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Susceptibility to HLA-DM protein is determined by a dynamic conformation of major histocompatibility complex class II molecule bound with peptide. | LitMetric

AI Article Synopsis

  • HLA-DM plays a crucial role in replacing weak peptides bound to MHCII molecules during the immune response, but the specific mechanism behind this process is still debated.
  • Research showed that peptides that bind poorly in the P1 pocket have less affinity for MHCII and are more easily exchanged by HLA-DM, with various experiments confirming structural changes during this process.
  • Interestingly, modifying certain residues can reverse these changes, and mutations outside the typical binding sites can further increase the likelihood of peptide exchange, suggesting that MHCII's overall flexibility is more important than just the occupancy of the P1 pocket.

Article Abstract

HLA-DM mediates the exchange of peptides loaded onto MHCII molecules during antigen presentation by a mechanism that remains unclear and controversial. Here, we investigated the sequence and structural determinants of HLA-DM interaction. Peptides interacting nonoptimally in the P1 pocket exhibited low MHCII binding affinity and kinetic instability and were highly susceptible to HLA-DM-mediated peptide exchange. These changes were accompanied by conformational alterations detected by surface plasmon resonance, SDS resistance assay, antibody binding assay, gel filtration, dynamic light scattering, small angle x-ray scattering, and NMR spectroscopy. Surprisingly, all of those changes could be reversed by substitution of the P9 pocket anchor residue. Moreover, MHCII mutations outside the P1 pocket and the HLA-DM interaction site increased HLA-DM susceptibility. These results indicate that a dynamic MHCII conformational determinant rather than P1 pocket occupancy is the key factor determining susceptibility to HLA-DM-mediated peptide exchange and provide a molecular mechanism for HLA-DM to efficiently target unstable MHCII-peptide complexes for editing and exchange those for more stable ones.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4156084PMC
http://dx.doi.org/10.1074/jbc.M114.585539DOI Listing

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